研究进展, 更新时间: 2005年11月10日
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低氧通过Notch信号维持细胞的不分化状态
2005-11-10
  

在发育中, 氧水平调控细胞增殖, 分化, 迁移, 和最终的器官形成。Gustaffson 等最新揭示, 低氧因子HIF-1调节Notch, 进而抑制细胞分化, 促进细胞增殖. 这一发现揭示了氧调控细胞分化的重要分子机理.


Dev Cell. 2005 Nov;9(5):617-28.

Hypoxia requires notch signaling to maintain the undifferentiated cell state.

Gustafsson MV, Zheng X, Pereira T, Gradin K, Jin S, Lundkvist J, Ruas JL, Poellinger L, Lendahl U, Bondesson M.

In addition to controlling a switch to glycolytic metabolism and induction of erythropoiesis and angiogenesis, hypoxia promotes the undifferentiated cell state in various stem and precursor cell populations. Here, we show that the latter process requires Notch signaling. Hypoxia blocks neuronal and myogenic differentiation in a Notch-dependent manner. Hypoxia activates Notch-responsive promoters and increases expression of Notch direct downstream genes. The Notch intracellular domain interacts with HIF-1alpha, a global regulator of oxygen homeostasis, and HIF-1alpha is recruited to Notch-responsive promoters upon Notch activation under hypoxic conditions. Taken together, these data provide molecular insights into how reduced oxygen levels control the cellular differentiation status and demonstrate a role for Notch in this process.


 

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